Modeling human pancreatic beta cell dedifferentiation

  • Marc Diedisheim
  • Masaya Oshima
  • Olivier Albagli
  • Charlotte Wennberg Huldt
  • Ingela Ahlstedt
  • Maryam Clausen
  • Suraj Menon
  • Alexander Aivazidis
  • Anne-Christine Andreasson
  • William G. Haynes
  • Piero Marchetti
  • Lorella Marselli
  • Mathieu Armanet
  • Fabrice Chimienti
  • Raphael Scharfmann
Publication date
April 2018
Publisher
Elsevier
ISSN
2212-8778
Journal
2212-8778

Abstract

Objective: Dedifferentiation could explain reduced functional pancreatic β-cell mass in type 2 diabetes (T2D). Methods: Here we model human β-cell dedifferentiation using growth factor stimulation in the human β-cell line, EndoC-βH1, and human pancreatic islets. Results: Fibroblast growth factor 2 (FGF2) treatment reduced expression of β-cell markers, (INS, MAFB, SLC2A2, SLC30A8, and GCK) and activated ectopic expression of MYC, HES1, SOX9, and NEUROG3. FGF2-induced dedifferentiation was time- and dose-dependent and reversible upon wash-out. Furthermore, FGF2 treatment induced expression of TNFRSF11B, a decoy receptor for RANKL and protected β-cells against RANKL signaling. Finally, analyses of transcriptomic data revealed increased FGF2 ex...

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